| Literature DB >> 32755586 |
Aria Vaishnavi1, Michael T Scherzer2, Conan G Kinsey3, Gennie L Parkman2, Amanda Truong2, Phaedra Ghazi2, Sophia Schuman1, Benjamin Battistone1, Ignacio Garrido-Laguna3, Martin McMahon4.
Abstract
NTRK1 gene fusions are actionable drivers of numerous human malignancies. Here, we show that expression of the TPR-NTRK1 fusion kinase in immortalized mouse pancreatic ductal epithelial (IMPE) (pancreas) or mouse lung epithelial (MLE-12) cells is sufficient to promote rapidly growing tumors in mice. Both tumor models are exquisitely sensitive to targeted inhibition with entrectinib, a tropomyosin-related kinase A (TRKA) inhibitor. Initial regression of NTRK1-driven tumors is driven by induced expression of BIM, such that BIM silencing leads to a diminished response to entrectinib in vivo. However, the emergence of drug-resistant disease limits the long-term durability of responses. Based on the reactivation of RAF>MEK>ERK signaling observed in entrectinib-treated tumors, we show that the combination of entrectinib plus the MEK1/2 inhibitor cobimetinib dramatically forestalls the onset of drug resistance in vivo. Collectively, these data provide a mechanistic rationale for rapid clinical deployment of combined inhibition of TRKA plus MEK1/2 in NTRK1-driven cancers.Entities:
Keywords: NTRK gene fusion; colorectal cancer; kinase oncoproteins; lung cancer; pancreatic cancer; pathway-targeted therapies
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Year: 2020 PMID: 32755586 PMCID: PMC7478141 DOI: 10.1016/j.celrep.2020.107994
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423